E" mul'markörtest för återfallsrisk e2er bröstbevarande kirurgi för duktal bröstcancer in situ (DCIS) Fredrik Wärnberg, Madeleine Wärnberg, Troy

E" mul'markörtest för återfallsrisk e2er bröstbevarande kirurgi för duktal bröstcancer in situ (DCIS) Fredrik Wärnberg, Madeleine Wärnberg, Troy Bremer, Pat Whitworth, Rakesh Patel, Todd Barry, Steven Linke, Stephen Lyle, Karl Simin, Wenjing Zhou, Karin Jirström Akademiska sjukhuset, Uppsala, Prelude Corp. Laguna Hills, Nashville Breast Center, Nashville, Good Samaritan Cancer Center, Los Gatos, Spectrum Pathology, Mission Viejo, University of MassachusePs, U.S.A., Lunds universitet, Patologkliniken, Lund

Bakgrund DCIS god prognos för överlevnad Lokala återfall 32% exer 20 år Radioterapi minskar lokala återfall med 50% Rela[v riskminskning gäller alla undergrupper Lågrisk SweDCIS RT(-) 20% lokala återfall

Bakgrund Cumulative incidence 0.4 0.3 0.2 0.1 A RT Gray's test, P = <0.001 Control 0 No. At Risk 0 2 4 6 8 10 12 14 16 18 20 Time (years) RT 526 521 512 502 487 475 469 462 448 435 422 Control 520 502 468 446 422 407 394 382 370 358 350 Cumulative incidence 0.4 0.3 0.2 0.1 B RT Invasive In situ Cumulative incidence 0.4 0.3 0.2 0.1 C Control 0 0 0 4 8 12 16 20 Time (years) 0 4 8 12 16 20 Time (years)

Mål Iden[fiera en lågriskgrupp som inte behöver strålbehandling

Pa'enter och Metod Två kohorter Uppsala/Västerås 1986-2004, n=354, DCIS, bröstbevarande kirurgi +/- RT, follow-up 12,2 år University of MassachusePs 1997-2006, n=296, DCIS, bröstbevarande kirurgi +/- RT, follow-up 7,2 år Endpoints Invasiva lokala återfall Alla lokala återfall (invasiva + DCIS)

Pa'enter och Metod Tumörmarkörer HER2, PgR, Ki-67, COX2, p16/ink4a, FOXA1, SIAH2 Kliniska faktorer Ålder, storlek, marginal, palpabel Sta[s[sk modell MulJpel n-fold cross validajon med en pre-definierad sta[s[sk analysplan för ap förutse förväntat ujall i prak[ken

Återfallsrisk e2er 10 år Invasiva återfall resp. Alla återfall BCS utan strålning BCS med strålning 95% CI Prevalens n 95% CI Prevalens n Invasiva Lågrisk 4% ±3% 70% 184 5% ±4% 71% 242 Invasiva Högrisk 30% ±11% 30% 80 6% ±6% 29% 97 Alla Lågrisk 8% ±6% 36% 95 7% ±6% 45% 153 Alla Högrisk 32% ±8% 64% 169 15% ±6% 55% 186

Återfallsrisk e2er 10 år Invasiva återfall resp. Alla återfall BCS utan strålning BCS med strålning 95% CI Prevalens n 95% CI Prevalens n Invasiva Lågrisk 4% ±3% 70% 184 5% ±4% 71% 242 Invasiva Högrisk 30% ±11% 30% 80 6% ±6% 29% 97 Alla Lågrisk 8% ±6% 36% 95 7% ±6% 45% 153 Alla Högrisk 32% ±8% 64% 169 15% ±6% 55% 186

Återfallsrisk e2er 10 år Invasiva återfall resp. Alla återfall BCS utan strålning BCS med strålning 95% CI Prevalens n 95% CI Prevalens n Invasiva Lågrisk 4% ±3% 70% 184 5% ±4% 71% 242 Invasiva Högrisk 30% ±11% 30% 80 6% ±6% 29% 97 Alla Lågrisk 8% ±6% 36% 95 7% ±6% 45% 153 Alla Högrisk 32% ±8% 64% 169 15% ±6% 55% 186

Återfallsrisk e2er 10 år Invasiva återfall resp. Alla återfall BCS utan strålning BCS med strålning 95% CI Prevalens n 95% CI Prevalens n Invasiva Lågrisk 4% ±3% 70% 184 5% ±4% 71% 242 Invasiva Högrisk 30% ±11% 30% 80 6% ±6% 29% 97 Alla Lågrisk 8% ±6% 36% 95 7% ±6% 45% 153 Alla Högrisk 32% ±8% 64% 169 15% ±6% 55% 186

Slutsats Med mul[markörtestet kan vi iden[fiera en lågriskgrupp DCIS som inte har någon nypa av strålbehandling Testet bygger på immunhistokemi och kliniska parametrar Resultaten kommer valideras i flera kohorter, bl. a. SweDCIS Frågor? Tack!

Pa'enter och Metod The COX enzymes play a central role in the biosynthe[c pathway of prostanoids. COX-2 gene is upregulated during inflamma[on, hypoxia and in many cancers. The COX genes encode for enzymes that catalyse the conversion from arachidonic acid to prostaglandins. The increased expression of COX-2 in tumourigenesis is secondary to mul[ple ac[va[ons and as a response to growth factors and oncogenes, including those in the EGFR/HER2/RAS/MAP kinase pathway. Conversely, COX-2 is rarely expressed in normal [ssue. The tumor suppressor gene p16 (also called MTS1, CDKN2 and INK4A) is a cyclin-dependent kinase (CDK) inhibitor and a nega[ve cell cycle regulator. The inac[va[on of p16 appears to be a common event in many cancers. Several other func[ons of p16, including induc[on of apoptosis and senescence, have been correlated to p16's an[-tumor/an[-prolifera[on effects. p16 is able to induce apoptosis of tumor cells: Adenoviral-mediated expression of p16 (Adp16) inhibits ovarian cancer cell growth and causes apoptosis. Forkhead box A1 (FOXA1), is a tumor and stromal markers that recently have been proposed as predictors of local recurrence in invasive breast cancer. FOXA1 expression appears to be relevant in the sub-classifica[on of luminal/er posi[ve tumors into two sub-groups with different biological behavior and prognosis corresponding to the luminal A and luminal B classes, iden[fied by gene expression profiling studies. FOXA1 is expressed in close associa[on with ERα, encoding for transcrip[on factors with a plausible involvement in the ERα-mediated ac[on in breast cancer. FOXA1 has been thought to be a significant predictor of a good outcome in breast cancer. SIAH2 was one of the genes significantly related with response and progression-free survival. SIAH2 is an ubiqui[n E3 ligase which ubiqui[nates proteins for proteasomal-dependent degrada[on and has target proteins in the RAS and estrogen signaling pathway, DNA damage response, cell growth and differen[a[on, angiogenesis and hypoxia. Studies in breast cancer showed SIAH2 mainly in ER-posi[ve tumors. In addi[on, estrogens upregulated SIAH2 on both mrna and protein level by a rapid transcrip[onal response mediated by the ER. A posi[ve rela[onship between SIAH2 mrna and ER protein levels. SIAH2 protein levels were predominantly upregulated in ER-nega[ve breast cancer. They also observed increased SIAH2 protein expression during the transi[on of carcinoma in situ to invasive cancer and concluded that high SIAH2 protein expression is associated with an unfavorable survival. Increased SIAH2 mrna levels with a favorable disease outcome in pa[ents with ER-posi[ve primary breast cancer. A posi[ve associa[on between SIAH2 mrna and disease-free survival (DFS). As yet, it is unknown why SIAH2 protein and mrna levels have opposed prognos[c value in these heterogeneous tumor specimens.